论文信息 - Function and regulation of human copper-transporting ATPases.

Function and regulation of human copper-transporting ATPases.

Copper-transporting ATPases (Cu-ATPases) ATP7A and ATP7B are evolutionarily conserved polytopic membrane proteins with essential roles in human physiology. The Cu-ATPases are expressed in most tissues, and their transport activity is crucial for central nervous system development, liver function, connective tissue formation, and many other physiological processes. The loss of ATP7A or ATP7B function is associated with severe metabolic disorders, Menkes disease, and Wilson disease. In cells, the Cu-ATPases maintain intracellular copper concentration by transporting copper from the cytosol across cellular membranes. They also contribute to protein biosynthesis by delivering copper into the lumen of the secretory pathway where metal ion is incorporated into copper-dependent enzymes. The biosynthetic and homeostatic functions of Cu-ATPases are performed in different cell compartments; targeting to these compartments and the functional activity of Cu-ATPase are both regulated by copper. In recent years, significant progress has been made in understanding the structure, function, and regulation of these essential transporters. These studies raised many new questions related to specific physiological roles of Cu-ATPases in various tissues and complex mechanisms that control the Cu-ATPase function. This review summarizes current data on the structural organization and functional properties of ATP7A and ATP7B as well as their localization and functions in various tissues, and discusses the current models of regulated trafficking of human Cu-ATPases.

[1] M. Paterson,et al. A novel deletion mutation within the carboxyl terminus of the copper-transporting ATPase gene causes Wilson disease , 2000, Journal of the Neurological Sciences.

[2] I. Bertini,et al. Structural Basis for the Function of the N-terminal Domain of the ATPase CopA from Bacillus subtilis* , 2003, Journal of Biological Chemistry.

[3] M. Linder,et al. Effects of copper and ceruloplasmin on iron transport in the Caco 2 cell intestinal model. , 2002, The Journal of nutritional biochemistry.

[4] V. Malhotra,et al. Protein kinase D regulates basolateral membrane protein exit from trans-Golgi network , 2004, Nature Cell Biology.

[5] A. E. Rossi,et al. Sarcoplasmic reticulum: The dynamic calcium governor of muscle , 2006, Muscle & nerve.

[6] Alexandre Benmerah,et al. Studies on endocytic mechanisms of the Menkes copper-translocating P-type ATPase (ATP7A; MNK) – Endocytosis of the Menkes protein , 2004, Biometals.

[7] J. Winther,et al. Evidence that translation reinitiation leads to a partially functional Menkes protein containing two copper-binding sites. , 2006, American journal of human genetics.

[8] R. Portmann,et al. Purification and functional reconstitution of the human Wilson copper ATPase, ATP7B , 2005, FEBS letters.

[9] W. Cheung,et al. Characterization of a Thermophilic P-type Ag+/Cu+-ATPase from the ExtremophileArchaeoglobus fulgidus* , 2002, The Journal of Biological Chemistry.

[10] M. Linder,et al. Iron and copper homeostasis and intestinal absorption using the Caco2 cell model , 2003, Biometals.

[11] D. Stokes,et al. Role of metal-binding domains of the copper pump from Archaeoglobus fulgidus. , 2006, Biochemical and biophysical research communications.

[12] M. Schaefer,et al. Interaction of the copper chaperone HAH1 with the Wilson disease protein is essential for copper homeostasis. , 1999, Proceedings of the National Academy of Sciences of the United States of America.

[13] J. Mercer,et al. Defective copper-induced trafficking and localization of the Menkes protein in patients with mild and copper-treated classical Menkes disease. , 1999, Human molecular genetics.

[14] J. Kaplan,et al. N-terminal Domains of Human Copper-transporting Adenosine Triphosphatases (the Wilson’s and Menkes Disease Proteins) Bind Copper Selectively in Vivo and in Vitro with Stoichiometry of One Copper Per Metal-binding Repeat* , 1997, The Journal of Biological Chemistry.

[15] Copper uptake and intracellular distribution in the human intestinal Caco-2 cell line , 2000, Biometals.

[16] D. Winge,et al. Cox17 Is Functional When Tethered to the Mitochondrial Inner Membrane* , 2004, Journal of Biological Chemistry.

[17] B. Pépin,et al. [Treatment of Wilson's disease]. , 1968, Les Cahiers du College de medecine des hopitaux de Paris.

[18] I. Voskoboinik,et al. Understanding the mechanism and function of copper P-type ATPases. , 2002, Advances in protein chemistry.

[19] R. Klausner,et al. A novel di-leucine motif and a tyrosine-based motif independently mediate lysosomal targeting and endocytosis of CD3 chains , 1992, Cell.

[20] L. Braiterman,et al. NH2-terminal signals in ATP7B Cu-ATPase mediate its Cu-dependent anterograde traffic in polarized hepatic cells. , 2005, American journal of physiology. Gastrointestinal and liver physiology.

[21] T. Kawaguchi,et al. Role of ATP7B in biliary copper excretion in a human hepatoma cell line and normal rat hepatocytes. , 2000, Gastroenterology.

[22] A. Wernimont,et al. Binding of Copper(I) by the Wilson Disease Protein and Its Copper Chaperone* , 2004, Journal of Biological Chemistry.

[23] K. Ramos,et al. The Involvement of Copper Transporter in Lead-induced Oxidative Stress in Astroglia , 2005, Neurochemical Research.

[24] I. Bertini,et al. Structure of human Wilson protein domains 5 and 6 and their interplay with domain 4 and the copper chaperone HAH1 in copper uptake. , 2006, Proceedings of the National Academy of Sciences of the United States of America.

[25] S. Lutsenko,et al. X-ray Absorption Spectroscopy of the Copper Chaperone HAH1 Reveals a Linear Two-coordinate Cu(I) Center Capable of Adduct Formation with Exogenous Thiols and Phosphines* , 2003, Journal of Biological Chemistry.

[26] J. Mössner,et al. High prevalence of the H1069Q mutation in East German patients with Wilson disease: rapid detection of mutations by limited sequencing and phenotype-genotype analysis. , 2001, Journal of hepatology.

[27] I. Voskoboinik,et al. Functional Analysis of the N-terminal CXXC Metal-binding Motifs in the Human Menkes Copper-transporting P-type ATPase Expressed in Cultured Mammalian Cells* , 1999, The Journal of Biological Chemistry.

[28] Stuart K. Kim,et al. PDZ‐mediated interactions retain the epithelial GABA transporter on the basolateral surface of polarized epithelial cells , 1999, The EMBO journal.

[29] S. Prigge,et al. New insights into copper monooxygenases and peptide amidation: structure, mechanism and function , 2000, Cellular and Molecular Life Sciences CMLS.

[30] T. Glover,et al. Molecular structure of the Menkes disease gene (ATP7A). , 1995, Genomics.

[31] A. Martel,et al. The Cadmium Transport Sites of CadA, the Cd2+-ATPase from Listeria monocytogenes* , 2006, Journal of Biological Chemistry.

[32] E. D. Harris,et al. A Menkes P-type ATPase involved in copper homeostasis in the central nervous system of the rat. , 1997, Brain research. Molecular brain research.

[33] R. Dick,et al. Correction of cerebrospinal fluid copper in Menkes kinky hair disease. , 1991, Pediatric neurology.

[34] L. Que,et al. Copper-induced conformational changes in the N-terminal domain of the Wilson disease copper-transporting ATPase. , 2000, Biochemistry.

[35] P. Lockhart,et al. Expression of the Menkes gene homologue in mouse tissues lack of effect of copper on the mRNA levels , 1994, FEBS letters.

[36] S. Packman,et al. Expression and accumulation of lysyl oxidase, elastin, and type I procollagen in human Menkes and mottled mouse fibroblasts. , 1993, Archives of biochemistry and biophysics.

[37] L. Peltonen,et al. Abnormal copper metabolism and deficient lysyl oxidase activity in a heritable connective tissue disorder. , 1982, The Journal of clinical investigation.

[38] S. Horton,et al. Animal models of Menkes disease. , 1999, Advances in experimental medicine and biology.

[39] A. Monaco,et al. Characterization of the Menkes protein copper-binding domains and their role in copper-induced protein relocalization. , 1999, Human molecular genetics.

[40] C. Wijmenga,et al. The ubiquitously expressed MURR1 protein is absent in canine copper toxicosis. , 2003, Journal of hepatology.

[41] P. Lockhart,et al. Functional analysis and intracellular localization of the human menkes protein (MNK) stably expressed from a cDNA construct in Chinese hamster ovary cells (CHO-K1). , 1998, Human molecular genetics.

[42] P. Lockhart,et al. Ligand‐regulated transport of the Menkes copper P‐type ATPase efflux pump from the Golgi apparatus to the plasma membrane: a novel mechanism of regulated trafficking. , 1996, The EMBO journal.

[43] M. Linder,et al. Ceruloplasmin and Copper Transport During the Latter Part of Gestation in the Rat , 1993, Proceedings of the Society for Experimental Biology and Medicine. Society for Experimental Biology and Medicine.

[44] M. Ushio-Fukai,et al. Essential role for the Menkes ATPase in activation of extracellular superoxide dismutase: implication for vascular oxidative stress , 2006, FASEB journal : official publication of the Federation of American Societies for Experimental Biology.

[45] W. Friedrichs,et al. Human ceruloplasmin. Tissue-specific expression of transcripts produced by alternative splicing. , 1990, The Journal of biological chemistry.

[46] G. Multhaup,et al. Copper Depletion Down-regulates Expression of the Alzheimer's Disease Amyloid-β Precursor Protein Gene* , 2004, Journal of Biological Chemistry.

[47] D W Cox,et al. Role of the Copper-binding Domain in the Copper Transport Function of ATP7B, the P-type ATPase Defective in Wilson Disease* , 1999, The Journal of Biological Chemistry.

[48] D. Thiele,et al. Biochemical Characterization of the Human Copper Transporter Ctr1* , 2002, The Journal of Biological Chemistry.

[49] N. Sugawara,et al. Biliary excretion of copper, metallothionein, and glutathione into Long-Evans Cinnamon rats: a convincing animal model for Wilson disease. , 1995, Biochemical and molecular medicine.

[50] C. Bucci,et al. Endosomal trafficking of the Menkes copper ATPase ATP7A is mediated by vesicles containing the Rab7 and Rab5 GTPase proteins. , 2003, Experimental cell research.

[51] H. Kodama,et al. Clinical manifestations and treatment of Menkes disease and its variants , 1999, Pediatrics international : official journal of the Japan Pediatric Society.

[52] I. Voskoboinik,et al. Copper-regulated Trafficking of the Menkes Disease Copper ATPase Is Associated with Formation of a Phosphorylated Catalytic Intermediate* , 2002, The Journal of Biological Chemistry.

[53] Y. Kuo,et al. Copper transport protein (Ctr1) levels in mice are tissue specific and dependent on copper status. , 2006, The Journal of nutrition.

[54] E. Cauza,et al. Distribution of patients with Wilson disease carrying the H1069Q mutation in Austria. , 2000, Wiener klinische Wochenschrift.

[55] D. Glerum,et al. Mutagenesis Reveals a Specific Role for Cox17p in Copper Transport to Cytochrome Oxidase* , 2003, Journal of Biological Chemistry.

[56] M. Cooper,et al. Copper Specifically Regulates Intracellular Phosphorylation of the Wilson's Disease Protein, a Human Copper-transporting ATPase* , 2001, The Journal of Biological Chemistry.

[57] J. Mercer,et al. Correction of a mouse model of Menkes disease by the human Menkes gene. , 2006, Biochimica et biophysica acta.

[58] T. O’Halloran,et al. Activation of superoxide dismutases: putting the metal to the pedal. , 2006, Biochimica et biophysica acta.

[59] Christopher E. Jones,et al. Structure and metal binding studies of the second copper binding domain of the Menkes ATPase. , 2003, Journal of structural biology.

[60] J. Prohaska,et al. Copper Transport and Metabolism Are Normal in Aceruloplasminemic Mice* , 2001, The Journal of Biological Chemistry.

[61] S. Snyder,et al. A Novel Pineal Night-Specific ATPase Encoded by the Wilson Disease Gene , 1999, The Journal of Neuroscience.

[62] THE MENKES DISEASE PROTEIN BINDS COPPER VIA NOVEL 2-COORDINATE CU(I)-CYSTEINATES IN THE N-TERMINAL DOMAIN , 1998 .

[63] S. Lutsenko,et al. Copper transfer to the N-terminal domain of the Wilson disease protein (ATP7B): X-ray absorption spectroscopy of reconstituted and chaperone-loaded metal binding domains and their interaction with exogenous ligands. , 2004, Journal of inorganic biochemistry.

[64] A. Mitchell,et al. Lysyl oxidase and P-ATPase-7A expression during embryonic development in the rat. , 2000, Archives of biochemistry and biophysics.

[65] S. Lutsenko,et al. The Lys1010–Lys1325 Fragment of the Wilson's Disease Protein Binds Nucleotides and Interacts with the N-terminal Domain of This Protein in a Copper-dependent Manner* , 2001, The Journal of Biological Chemistry.

[66] T. Gilliam,et al. Null mutation of the murine ATP7B (Wilson disease) gene results in intracellular copper accumulation and late-onset hepatic nodular transformation. , 1999, Human molecular genetics.

[67] G. Mancini,et al. Mechanisms of Copper Incorporation into Human Ceruloplasmin* , 2002, The Journal of Biological Chemistry.

[68] T. Glover,et al. A novel frameshift mutation in exon 23 of ATP7A (MNK) results in occipital horn syndrome and not in Menkes disease. , 2001, American journal of human genetics.

[69] M. Reddy,et al. Pretranslational control of Menkes disease gene expression , 2003, Biometals.

[70] M. Linder,et al. Copper transport. , 1998, The American journal of clinical nutrition.

[71] A. Monaco,et al. Novel membrane traffic steps regulate the exocytosis of the Menkes disease ATPase. , 2002, Human molecular genetics.

[72] A. Angius,et al. Molecular characterization of Wilson disease in the Sardinian population—Evidence of a founder effect , 1999, Human mutation.

[73] G. Samimi,et al. Increased Expression of the Copper Efflux Transporter ATP7A Mediates Resistance to Cisplatin, Carboplatin, and Oxaliplatin in Ovarian Cancer Cells , 2004, Clinical Cancer Research.

[74] R. Mains,et al. Supplying Copper to the Cuproenzyme Peptidylglycine α-Amidating Monooxygenase* , 2003, The Journal of Biological Chemistry.

[75] P. Angus,et al. Diagnosis of Wilson's disease: an experience over three decades , 2000, Gut.

[76] Dominique L. Cosco,et al. The copper transporter CTR1 provides an essential function in mammalian embryonic development , 2001, Proceedings of the National Academy of Sciences of the United States of America.

[77] G. Shepherd,et al. Differential modulation by zinc and copper of amino acid receptors from rat olfactory bulb neurons. , 1996, Journal of neurophysiology.

[78] G. Multhaup,et al. Kinetic Analysis of the Interaction of the Copper Chaperone Atox1 with the Metal Binding Sites of the Menkes Protein* , 2003, Journal of Biological Chemistry.

[79] T. Dunn,et al. The Menkes/Wilson disease gene homologue in yeast provides copper to a ceruloplasmin-like oxidase required for iron uptake. , 1995, Proceedings of the National Academy of Sciences of the United States of America.

[80] J. Borjigin,et al. A new strain of rat for functional analysis of PINA. , 2005, Brain research. Molecular brain research.

[81] J. Kaplan,et al. Functional Properties of the Copper-transporting ATPase ATP7B (The Wilson's Disease Protein) Expressed in Insect Cells* , 2002, The Journal of Biological Chemistry.

[82] T. Gilliam,et al. Characterization of the Wilson disease gene encoding a P-type copper transporting ATPase: genomic organization, alternative splicing, and structure/function predictions. , 1994, Human molecular genetics.

[83] L. Vyklický,et al. Copper Modulation of NMDA Responses in Mouse and Rat Cultured Hippocampal Neurons , 1996, The European journal of neuroscience.

[84] I. Bertini,et al. Metallochaperones and metal-transporting ATPases: a comparative analysis of sequences and structures. , 2002, Genome research.

[85] R. Klausner,et al. Biochemical Characterization of the Wilson Disease Protein and Functional Expression in the Yeast Saccharomyces cerevisiae * , 1997, The Journal of Biological Chemistry.

[86] J. C. Wilkinson,et al. XIAP Is a copper binding protein deregulated in Wilson's disease and other copper toxicosis disorders. , 2006, Molecular cell.

[87] S. Packman,et al. A repeated element in the regulatory region of the MNK gene and its deletion in a patient with occipital horn syndrome. , 1996, Human molecular genetics.

[88] J. Gitlin,et al. The Role of Copper in Neurodegenerative Disease , 1999, Neurobiology of Disease.

[89] P. Avner,et al. Genomic organization of the mottled gene, the mouse homologue of the human Menkes disease gene. , 1996, Genomics.

[90] Jun-bo Liu,et al. Conserved aspartic acid 714 in transmembrane segment 8 of the ZntA subgroup of P1B-type ATPases is a metal-binding residue. , 2006, Biochemistry.

[91] M. Zastrow,et al. Cargo Regulates Clathrin-Coated Pit Dynamics , 2006, Cell.

[92] T. Kawaguchi,et al. Copper does not alter the intracellular distribution of ATP7B, a copper-transporting ATPase. , 2000, Biochemical and biophysical research communications.

[93] J. Forbes,et al. Identification of the "missing domain" of the rat copper-transporting ATPase, atp7b: insight into the structural and metal binding characteristics of its N-terminal copper-binding domain. , 2004, Biochimica et biophysica acta.

[94] S. Kaler. Diagnosis and therapy of Menkes syndrome, a genetic form of copper deficiency. , 1998, The American journal of clinical nutrition.

[95] I. Saatci,et al. Cranial MR findings in Wilson's disease , 1997, Acta radiologica.

[96] D. W. Neill,et al. The diagnosis and treatment of Wilson's disease. , 1958, Brain : a journal of neurology.

[97] M Qi,et al. Constitutive skipping of alternatively spliced exon 10 in the ATP7A gene abolishes Golgi localization of the menkes protein and produces the occipital horn syndrome. , 1998, Human molecular genetics.

[98] D. Cox,et al. Diagnosis and phenotypic classification of Wilson disease 1 , 2003, Liver international : official journal of the International Association for the Study of the Liver.

[99] Thomas W. Glover,et al. Isolation of a partial candidate gene for Menkes disease by positional cloning , 1993, Nature Genetics.

[100] G. Ronnett,et al. The Developmentally Regulated Expression of Menkes Protein ATP7A Suggests a Role in Axon Extension and Synaptogenesis , 2005, Developmental Neuroscience.

[101] Y. Kageyama,et al. MR of the base of the pons in Wilson disease. , 1992, AJNR. American journal of neuroradiology.

[102] J. Mercer,et al. The Menkes copper transporter is required for the activation of tyrosinase. , 2000, Human molecular genetics.

[103] R. Palmiter,et al. A murine model of Menkes disease reveals a physiological function of metallothionein , 1996, Nature Genetics.

[104] A. Monaco,et al. Characterization of the exon structure of the Menkes disease gene using vectorette PCR. , 1995, Genomics.

[105] S. Lutsenko,et al. Metallochaperone Atox1 Transfers Copper to the NH2-terminal Domain of the Wilson's Disease Protein and Regulates Its Catalytic Activity* , 2002, The Journal of Biological Chemistry.

[106] J. L. Durant,et al. Wilson's disease with reversible renal tubular dysfunction. Correlation with proximal tubular ultrastructure. , 1971, Annals of internal medicine.

[107] A. K. Mandal,et al. Identification of the Transmembrane Metal Binding Site in Cu+-transporting PIB-type ATPases* , 2004, Journal of Biological Chemistry.

[108] T. Bolin,et al. Diagnosis of Wilson ’ s disease : an experience over three decades , 2022 .

[109] M. Shimada,et al. Neuropathological study on cerebellum of macular mutant mouse heterozygote , 2004, Acta Neuropathologica.

[110] D. Thiele,et al. Essential role for mammalian copper transporter Ctr1 in copper homeostasis and embryonic development , 2001, Proceedings of the National Academy of Sciences of the United States of America.

[111] F. S. Mathews,et al. HAH1 Is a Copper-binding Protein with Distinct Amino Acid Residues Mediating Copper Homeostasis and Antioxidant Defense* , 1998, The Journal of Biological Chemistry.

[112] D. Dooley,et al. Human kidney diamine oxidase: heterologous expression, purification, and characterization , 2002, JBIC Journal of Biological Inorganic Chemistry.

[113] I. Voskoboinik,et al. ATP‐dependent copper transport by the Menkes protein in membrane vesicles isolated from cultured Chinese hamster ovary cells , 1998, FEBS letters.

[114] S. Packman,et al. Mutation Analysis and Expression of the Mottled Gene in the Macular Mouse Model of Menkes Disease , 1997, Pediatric Research.

[115] K. Allen,et al. Chronological changes in tissue copper, zinc and iron in the toxic milk mouse and effects of copper loading , 2006, Biometals.

[116] S. Packman,et al. Isolation of a candidate gene for Menkes disease and evidence that it encodes a copper–transporting ATPase , 1993, Nature Genetics.

[117] A. Wernimont,et al. Structural basis for copper transfer by the metallochaperone for the Menkes/Wilson disease proteins , 2000, Nature Structural Biology.

[118] G. Multhaup,et al. Copper in disorders with neurological symptoms: Alzheimer’s, Menkes, and Wilson diseases , 2001, Brain Research Bulletin.

[119] D. Cox,et al. Functional assessment of the carboxy-terminus of the Wilson disease copper-transporting ATPase, ATP7B. , 2004, Genomics.

[120] D. Goldstein,et al. Occipital horn syndrome and a mild Menkes phenotype associated with splice site mutations at the MNK locus , 1994, Nature Genetics.

[121] J. Gitlin,et al. Functional Expression of the Menkes Disease Protein Reveals Common Biochemical Mechanisms Among the Copper-transporting P-type ATPases* , 1998, The Journal of Biological Chemistry.

[122] C. Wijmenga,et al. The Copper Toxicosis Gene Product Murr1 Directly Interacts with the Wilson Disease Protein* , 2003, Journal of Biological Chemistry.

[123] S. Kaler,et al. Copper‐replacement treatment for symptomatic Menkes disease: ethical considerations , 2005, Clinical genetics.

[124] Yurij A. Kosinsky,et al. The Distinct Functional Properties of the Nucleotide-binding Domain of ATP7B, the Human Copper-transporting ATPase* , 2004, Journal of Biological Chemistry.

[125] J. Mercer,et al. Copper exposure induces trafficking of the menkes protein in intestinal epithelium of ATP7A transgenic mice. , 2005, The Journal of nutrition.

[126] T. Kawaguchi,et al. Wilson disease protein ATP7B is localized in the late endosomes in a polarized human hepatocyte cell line. , 2003, International journal of molecular medicine.

[127] D. Thiele,et al. Characterization of Mouse Embryonic Cells Deficient in the Ctr1 High Affinity Copper Transporter , 2002, The Journal of Biological Chemistry.

[128] J. Gitlin,et al. Mechanisms of copper incorporation during the biosynthesis of human ceruloplasmin. , 1991, The Journal of biological chemistry.

[129] A. Craig,et al. NMDA Receptor Activation Mediates Copper Homeostasis in Hippocampal Neurons , 2005, The Journal of Neuroscience.

[130] Min-ting Lin,et al. Molecular diagnosis and prophylactic therapy for presymptomatic Chinese patients with Wilson disease. , 2003, Archives of neurology.

[131] M. Nishimura,et al. A serine-to-proline mutation in the copper-transporting P-type ATPase gene of the macular mouse , 1997, Mammalian Genome.

[132] Renu M. Stephen,et al. Menkes Copper ATPase (Atp7a) Is a Novel Metal-responsive Gene in Rat Duodenum, and Immunoreactive Protein Is Present on Brush-border and Basolateral Membrane Domains* , 2005, Journal of Biological Chemistry.

[133] P. Lockhart,et al. Correction of the Copper Transport Defect of Menkes Patient Fibroblasts by Expression of the Menkes and Wilson ATPases* , 1998, The Journal of Biological Chemistry.

[134] G. Samimi,et al. The copper export pump ATP7B modulates the cellular pharmacology of carboplatin in ovarian carcinoma cells. , 2003, Molecular pharmacology.

[135] M. Knöpfel,et al. ATP-driven copper transport across the intestinal brush border membrane. , 2005, Biochemical and biophysical research communications.

[136] Ya Hui Hung,et al. Purification and membrane reconstitution of catalytically active Menkes copper-transporting P-type ATPase (MNK; ATP7A). , 2007, The Biochemical journal.

[137] S. Weinman,et al. Involvement of chloride channels in hepatic copper metabolism: ClC-4 promotes copper incorporation into ceruloplasmin. , 2004, Gastroenterology.

[138] J. Gitlin,et al. Ceruloplasmin gene expression in the murine central nervous system. , 1996, The Journal of clinical investigation.

[139] T. Sugiyama,et al. Restoration of Holoceruloplasmin Synthesis in LEC Rat after Infusion of Recombinant Adenovirus Bearing WND cDNA* , 1998, The Journal of Biological Chemistry.

[140] G. Jansen,et al. Cranial MR in Wilson disease: abnormal white matter in extrapyramidal and pyramidal tracts. , 1995, AJNR. American journal of neuroradiology.

[141] J. Mercer,et al. Copper-dependent interaction of glutaredoxin with the N termini of the copper-ATPases (ATP7A and ATP7B) defective in Menkes and Wilson diseases. , 2006, Biochemical and biophysical research communications.

[142] R. Parton,et al. Effect of the toxic milk mutation (tx) on the function and intracellular localization of Wnd, the murine homologue of the Wilson copper ATPase. , 2001, Human molecular genetics.

[143] Jun-bo Liu,et al. Kinetic analysis of metal binding to the amino-terminal domain of ZntA by monitoring metal-thiolate charge-transfer complexes. , 2005, Biochemistry.

[144] T. Glant,et al. Common mutations of ATP7B in Wilson disease patients from Hungary. , 2002, American journal of medical genetics.

[145] D. Radisky,et al. Chloride is an allosteric effector of copper assembly for the yeast multicopper oxidase Fet3p: an unexpected role for intracellular chloride channels. , 1998, Proceedings of the National Academy of Sciences of the United States of America.

[146] M. Schaefer,et al. IV. Wilson's disease and Menkes disease. , 1999, American journal of physiology. Gastrointestinal and liver physiology.

[147] M. Petris. The SLC31 (Ctr) copper transporter family , 2004, Pflügers Archiv.

[148] A. Algra,et al. Wilson disease: findings at MR imaging and CT of the brain with clinical correlation. , 1996, Radiology.

[149] M. Hirose,et al. Dynamic mechanism for the serpin loop insertion as revealed by quantitative kinetics. , 2005, Journal of molecular biology.

[150] R. Klein,et al. Cultured astrocytes express mRNA for peptidylglycine-α-amidating monooxygenase, a neuropeptide processing enzyme , 1992, Brain Research.

[151] H. Kodama,et al. Molecular genetics and pathophysiology of Menkes disease , 1999, Pediatrics international : official journal of the Japan Pediatric Society.

[152] S. Arya,et al. Neuronal and vascular disorders of the brain and spinal cord in Menkes kinky hair disease. , 1987, American journal of medical genetics. Supplement.

[153] R. Vonk,et al. Copper-induced apical trafficking of ATP7B in polarized hepatoma cells provides a mechanism for biliary copper excretion. , 2000, Gastroenterology.

[154] A. Monaco,et al. A Golgi localization signal identified in the Menkes recombinant protein. , 1998, Human molecular genetics.

[155] J. Mercer,et al. Copper binding to the N-terminal metal-binding sites or the CPC motif is not essential for copper-induced trafficking of the human Wilson protein (ATP7B). , 2007, The Biochemical journal.

[156] J. Gitlin,et al. Essential role for Atox1 in the copper-mediated intracellular trafficking of the Menkes ATPase , 2003, Proceedings of the National Academy of Sciences of the United States of America.

[157] T. Hosokawa,et al. Immunohistochemical determination of the Wilson Copper-transporting P-type ATPase in the brain tissues of the rat , 1999, Neuroscience Letters.

[158] C. Rensing,et al. The ATP Hydrolytic Activity of Purified ZntA, a Pb(II)/Cd(II)/Zn(II)-translocating ATPase from Escherichia coli * , 2000, The Journal of Biological Chemistry.

[159] M. Schaefer,et al. IV. Wilson's disease and Menkes disease. , 1999, American journal of physiology. Gastrointestinal and liver physiology.

[160] Kinuko Suzuki,et al. Abnormalities of Purkinje Cell Arborization in Brindled Mouse Cerebellum: A Golgi Study , 1985, Journal of neuropathology and experimental neurology.

[161] S. Kaler,et al. Downregulation of myelination, energy, and translational genes in Menkes disease brain. , 2005, Molecular genetics and metabolism.

[162] Y. Kuroiwa,et al. CT manifestation of cerebral white matter lesion in Wilson disease , 1983, Annals of neurology.

[163] D. Cox,et al. Expression, Purification, and Metal Binding Properties of the N-terminal Domain from the Wilson Disease Putative Copper-transporting ATPase (ATP7B)* , 1997, The Journal of Biological Chemistry.

[164] S. Kaler,et al. Severe bilateral panlobular emphysema and pulmonary arterial hypoplasia: Unusual manifestations of Menkes disease , 2005, American journal of medical genetics. Part A.

[165] S. Kelleher,et al. Mammary gland copper transport is stimulated by prolactin through alterations in Ctr1 and Atp7A localization. , 2006, American journal of physiology. Regulatory, integrative and comparative physiology.

[166] M. Harada,et al. Wilson disease , 2002, Medical Electron Microscopy.

[167] M. Knöpfel,et al. Characterization of a Cytochrome b558 Ferric/Cupric Reductase from Rabbit Duodenal Brush Border Membranes , 2002 .

[168] Alexandre M J J Bonvin,et al. A docking approach to the study of copper trafficking proteins; interaction between metallochaperones and soluble domains of copper ATPases. , 2004, Structure.

[169] G. Kreitzer,et al. cdc42 regulates the exit of apical and basolateral proteins from the trans‐Golgi network , 2001, The EMBO journal.

[170] T. Glover,et al. Immunocytochemical Localization of the Menkes Copper Transport Protein (ATP7A) to the Trans-Golgi Network , 1997, Human molecular genetics.

[171] J. Mercer,et al. The Menkes protein (ATP7A; MNK) cycles via the plasma membrane both in basal and elevated extracellular copper using a C-terminal di-leucine endocytic signal. , 1999, Human molecular genetics.

[172] S. Lutsenko,et al. The Copper-transporting ATPases, Menkes and Wilson Disease Proteins, Have Distinct Roles in Adult and Developing Cerebellum* , 2005, Journal of Biological Chemistry.

[173] M. Reddy,et al. Coincident expression of Menkes gene with copper efflux in human placental cells. , 1996, The American journal of physiology.

[174] N. Bonander,et al. Cooperative binding of copper(I) to the metal binding domains in Menkes disease protein. , 1999, Biochimica et biophysica acta.

[175] W. Stremmel,et al. [Therapy of Wilson disease]. , 1999, Zeitschrift fur Gastroenterologie.

[176] P. Gruss,et al. The metallochaperone Atox1 plays a critical role in perinatal copper homeostasis , 2001, Proceedings of the National Academy of Sciences of the United States of America.

[177] E. J. Cornish,et al. Expression of Menkes disease gene in mammary carcinoma cells. , 1997, The Biochemical journal.

[178] M. Knöpfel,et al. Characterization of a cytochrome b(558) ferric/cupric reductase from rabbit duodenal brush border membranes. , 2002, Biochemical and biophysical research communications.

[179] Mariko Suzuki1 and Jonathan D Gitlin. Intracellular localization of the Menkes and Wilson’s disease proteins and their role in intracellular copper transport , 1999, Pediatrics international : official journal of the Japan Pediatric Society.

[180] M. Núñez,et al. DMT1, a physiologically relevant apical Cu1+ transporter of intestinal cells. , 2003, American journal of physiology. Cell physiology.

[181] R. Mains,et al. Menkes Protein Contributes to the Function of Peptidylglycine α-Amidating Monooxygenase , 2003, Endocrinology.

[182] William I. Wood,et al. Solution structure of the fourth metal-binding domain from the Menkes copper-transporting ATPase , 1998, Nature Structural Biology.

[183] H. Ushijima,et al. ATP7A gene mutations in 16 patients with Menkes disease and a patient with occipital horn syndrome. , 2001, American journal of medical genetics.

[184] A. Rosato,et al. Solution structure of the apo and copper(I)-loaded human metallochaperone HAH1. , 2004, Biochemistry.

[185] R. Mains,et al. Supplying copper to the cuproenzyme peptidylglycine alpha-amidating monooxygenase. , 2003, The Journal of biological chemistry.

[186] C. Rensing,et al. Escherichia coli CopA N-terminal Cys(X)(2)Cys motifs are not required for copper resistance or transport. , 2001, Biochemical and biophysical research communications.

[187] S. Lutsenko,et al. A Mutation in the ATP7B Copper Transporter Causes Reduced Dopamine β-Hydroxylase and Norepinephrine in Mouse Adrenal , 2003, Neurochemical Research.

[188] J. Mercer,et al. A Single PDZ Domain Protein Interacts with the Menkes Copper ATPase, ATP7A , 2005, Journal of Biological Chemistry.

[189] W. R. Lieb,et al. The two-pore-domain K(+) channels TREK-1 and TASK-3 are differentially modulated by copper and zinc. , 2004, Molecular Pharmacology.

[190] B. Nichols,et al. Flotillin-1 defines a clathrin-independent endocytic pathway in mammalian cells , 2006, Nature Cell Biology.

[191] D. Nolde,et al. Molecular modelling of the nucleotide-binding domain of Wilson's disease protein: location of the ATP-binding site, domain dynamics and potential effects of the major disease mutations. , 2004, The Biochemical journal.

[192] B. Sarkar,et al. Copper transport and its defect in Wilson disease: characterization of the copper-binding domain of Wilson disease ATPase. , 2000, Journal of inorganic biochemistry.

[193] J. Collins,et al. Identification of differentially expressed genes in response to dietary iron deprivation in rat duodenum. , 2005, American journal of physiology. Gastrointestinal and liver physiology.

[194] R. Dwek,et al. Tyrosinase folding and copper loading in vivo: a crucial role for calnexin and alpha-glucosidase II. , 1999, Biochemical and biophysical research communications.

[195] Cloning and characterization of the promoter region of the Wilson disease gene. , 1999, Biochemical and biophysical research communications.

[196] I. Voskoboinik,et al. Copper stimulates trafficking of a distinct pool of the Menkes copper ATPase (ATP7A) to the plasma membrane and diverts it into a rapid recycling pool. , 2004, The Biochemical journal.

[197] T. Aoki. Wilson's disease and Menkes disease. , 1999, Pediatrics international : official journal of the Japan Pediatric Society.

[198] K. Bissig,et al. Expression of the Human Menkes ATPase in Xenopus laevis Oocytes , 2001, Biological chemistry.

[199] J. Gitlin,et al. Ceruloplasmin metabolism and function. , 2002, Annual review of nutrition.

[200] P. Hedera,et al. Treatment of Wilson Disease With Ammonium Tetrathiomolybdate: III. Initial Therapy in a Total of 55 Neurologically Affected Patients and Follow-up With Zinc Therapy , 1996 .

[201] S. Lutsenko,et al. The Distinct Roles of the N-terminal Copper-binding Sites in Regulation of Catalytic Activity of the Wilson's Disease Protein* , 2003, Journal of Biological Chemistry.

[202] D. Winge,et al. Specific Copper Transfer from the Cox17 Metallochaperone to Both Sco1 and Cox11 in the Assembly of Yeast Cytochrome c Oxidase* , 2004, Journal of Biological Chemistry.

[203] Sebasián Mana-Capelli,et al. Archaeoglobus fulgidus CopB Is a Thermophilic Cu2+-ATPase , 2003, Journal of Biological Chemistry.

[204] J. Brunberg,et al. Treatment of Wilson disease with ammonium tetrathiomolybdate. II. Initial therapy in 33 neurologically affected patients and follow-up with zinc therapy. , 1996, Archives of neurology.

[205] A. Rosenzweig,et al. Structure of the actuator domain from the Archaeoglobus fulgidus Cu(+)-ATPase. , 2006, Biochemistry.

[206] N. Yoshimura,et al. Histochemical localization of copper in various organs of brindled mice after copper therapy , 1995, Pathology international.

[207] C. Wijmenga,et al. A novel role for XIAP in copper homeostasis through regulation of MURR1 , 2004, The EMBO journal.

[208] M. Schaefer,et al. Hepatocyte-specific localization and copper-dependent trafficking of the Wilson's disease protein in the liver. , 1999, The American journal of physiology.

[209] D. Thiele,et al. Ctr1 drives intestinal copper absorption and is essential for growth, iron metabolism, and neonatal cardiac function. , 2006, Cell metabolism.

[210] J. Camakaris,et al. A C-terminal di-leucine is required for localization of the Menkes protein in the trans-Golgi network. , 1998, Human molecular genetics.

[211] S. Packman,et al. Deletion of the promoter region in the Atp7a gene of the mottled dappled mouse , 1997, Nature Genetics.

[212] J. Mercer,et al. Copper-induced trafficking of the Cu-ATPases: A key mechanism for copper homeostasis , 2003, Biometals.

[213] I. Voskoboinik,et al. Signals regulating trafficking of Menkes (MNK; ATP7A) copper-translocating P-type ATPase in polarized MDCK cells. , 2004, American journal of physiology. Cell physiology.

[214] P. Krajacic,et al. Retinal localization and copper-dependent relocalization of the Wilson and Menkes disease proteins. , 2006, Investigative ophthalmology & visual science.

[215] Z. Tümer,et al. Menkes disease: Underlying genetic defect and new diagnostic possibilities , 1998, Journal of Inherited Metabolic Disease.

[216] T. Sugiyama,et al. Analysis of functional domains of Wilson disease protein (ATP7B) in Saccharomyces cerevisiae , 1998, FEBS letters.

[217] H. Sugimura,et al. Localization of Menkes gene expression in the mouse brain; its association with neurological manifestations in Menkes model mice , 1996, Acta Neuropathologica.

[218] H. Kodama. Recent developments in Menkes disease , 1993, Journal of Inherited Metabolic Disease.

[219] I. Voskoboinik,et al. The Regulation of Catalytic Activity of the Menkes Copper-translocating P-type ATPase , 2001, The Journal of Biological Chemistry.

[220] Christos T. Chasapis,et al. An NMR study of the interaction between the human copper(I) chaperone and the second and fifth metal‐binding domains of the Menkes protein , 2005, The FEBS journal.

[221] D. Holtzman,et al. Role of the Menkes copper-transporting ATPase in NMDA receptor-mediated neuronal toxicity , 2006, Proceedings of the National Academy of Sciences.

[222] Anthony P. Monaco,et al. Isolation of a candidate gene for Menkes disease that encodes a potential heavy metal binding protein , 1993, Nature Genetics.

[223] A. Monaco,et al. The Menkes disease ATPase (ATP7A) is internalized via a Rac1-regulated, clathrin- and caveolae-independent pathway. , 2003, Human molecular genetics.

[224] J. Prohaska,et al. Intracellular copper transport in mammals. , 2004, The Journal of nutrition.

[225] H. Kretzschmar,et al. Synapse Formation and Function Is Modulated by the Amyloid Precursor Protein , 2006, The Journal of Neuroscience.

[226] M. Mutoh,et al. Copper-transporting P-type adenosine triphosphatase (ATP7B) is associated with cisplatin resistance. , 2000, Cancer research.

[227] A. Rosato,et al. The Atx1-Ccc2 complex is a metal-mediated protein-protein interaction , 2006, Nature chemical biology.

[228] P. Ferenci. Review article: diagnosis and current therapy of Wilson's disease. , 2004, Alimentary pharmacology & therapeutics.

[229] P. Anikijenko,et al. Expression of Menkes Copper-transporting ATPase, MNK, in the Lactating Human Breast: Possible Role in Copper Transport into Milk , 1999, The journal of histochemistry and cytochemistry : official journal of the Histochemistry Society.

[230] S. Packman,et al. Developmental expression of the mouse mottled and toxic milk genes suggests distinct functions for the Menkes and Wilson disease copper transporters. , 1997, Human molecular genetics.

[231] D. Cox,et al. Intracellular trafficking of the human Wilson protein: the role of the six N-terminal metal-binding sites. , 2004, The Biochemical journal.

[232] H. Kodama,et al. Mottled gene expression and copper distribution in the macular mouse, an animal model for Menkes disease , 1998, Journal of Inherited Metabolic Disease.

[233] Z. Tümer,et al. Menkes disease: recent advances and new insights into copper metabolism. , 1996, Annals of medicine.

[234] D. Danks,et al. Copper metabolism in mottled mouse mutants: copper therapy of brindled (Mobr) mice. , 1979, The Biochemical journal.

[235] E. Wallace,et al. Expression and localization of menkes and Wilson copper transporting ATPases in human placenta. , 2004, Placenta.

[236] A. P. Einholm,et al. Glutamate-183 in the conserved TGES motif of domain A of sarcoplasmic reticulum Ca2+-ATPase assists in catalysis of E2/E2P partial reactions. , 2004, Proceedings of the National Academy of Sciences of the United States of America.

[237] J. Mercer,et al. Copper-dependent Interaction of Dynactin Subunit p62 with the N Terminus of ATP7B but Not ATP7A* , 2006, Journal of Biological Chemistry.

[238] D. Alberts,et al. Increase in expression of the copper transporter ATP7A during platinum drug-based treatment is associated with poor survival in ovarian cancer patients. , 2003, Clinical cancer research : an official journal of the American Association for Cancer Research.

[239] M. Linder,et al. Transcuprein is a macroglobulin regulated by copper and iron availability. , 2007, The Journal of nutritional biochemistry.

[240] R. Spritz,et al. Mutational analysis of copper binding by human tyrosinase. , 1997, The Journal of investigative dermatology.

[241] Recent advances in intestinal iron transport , 2005, Current gastroenterology reports.

[242] T. Gilliam,et al. Characterization of the Interaction between the Wilson and Menkes Disease Proteins and the Cytoplasmic Copper Chaperone, HAH1p* , 1999, The Journal of Biological Chemistry.

[243] K. Allen,et al. Defective localization of the Wilson disease protein (ATP7B) in the mammary gland of the toxic milk mouse and the effects of copper supplementation. , 2000, The Biochemical journal.

[244] A. Mitchell,et al. Copper, lysyl oxidase, and extracellular matrix protein cross-linking. , 1998, The American journal of clinical nutrition.

[245] O. Yoo,et al. Nuclear proteins that bind to metal response element a (MREa) in the Wilson disease gene promoter are Ku autoantigens and the Ku-80 subunit is necessary for basal transcription of the WD gene. , 2002, European journal of biochemistry.

[246] I. Voskoboinik,et al. Mutational analysis of the Menkes copper P-type ATPase (ATP7A). , 2003, Biochemical and biophysical research communications.

[247] T. Furuyama,et al. Expression of copper trafficking genes in the mouse brain , 1998, Neuroreport.

[248] G. Brewer,et al. Treatment of Wilson's Disease , 1987, Seminars in neurology.

[249] Jingshi Wu,et al. The LEC rat has a deletion in the copper transporting ATPase gene homologous to the Wilson disease gene , 1994, Nature Genetics.

[250] T. Hosokawa,et al. Histochemical characterization of silver-induced metallothionein in rat kidney. , 2000, Journal of inorganic biochemistry.

[251] P. Lockhart,et al. Molecular basis of the brindled mouse mutant (Mo(br)): a murine model of Menkes disease. , 1997, Human molecular genetics.

[252] G. Veglia,et al. Solution structures of the reduced and Cu(I) bound forms of the first metal binding sequence of ATP7A associated with Menkes disease , 2005, Proteins.

[253] J. Peppercorn,et al. The Wilson disease gene is a copper transporting ATPase with homology to the Menkes disease gene , 1993, Nature Genetics.

[254] S H Snyder,et al. A pineal regulatory element (PIRE) mediates transactivation by the pineal/retina-specific transcription factor CRX. , 1998, Proceedings of the National Academy of Sciences of the United States of America.

[255] Golgi study on macular mutant mouse after copper therapy , 2004, Acta Neuropathologica.

[256] J. Argüello. Identification of Ion-Selectivity Determinants in Heavy-Metal Transport P1B-type ATPases , 2003, The Journal of Membrane Biology.

[257] F. Hajós,et al. Nerve endings from rat brain tissue release copper upon depolarization. A possible role in regulating neuronal excitability , 1989, Neuroscience Letters.

[258] S Lutsenko,et al. The Wilson's disease protein expressed in Sf9 cells is phosphorylated. , 2001, Biochemical Society transactions.

[259] R. Pearson,et al. Protein kinase-dependent phosphorylation of the Menkes copper P-type ATPase. , 2003, Biochemical and biophysical research communications.

[260] J. Camakaris,et al. Hormonal regulation of the Menkes and Wilson copper-transporting ATPases in human placental Jeg-3 cells. , 2007, The Biochemical journal.

[261] J. Mercer,et al. Molecular and cellular aspects of copper transport in developing mammals. , 2003, The Journal of nutrition.

[262] M. Linder,et al. Vesicular transport of fe and interaction with other metal ions in polarized Caco2 cell monolayers. , 2006, Biological research.

[263] D W Cox,et al. The toxic milk mouse is a murine model of Wilson disease. , 1996, Human molecular genetics.

[264] I. Voskoboinik,et al. Functional studies on the Wilson copper P-type ATPase and toxic milk mouse mutant. , 2001, Biochemical and biophysical research communications.

[265] E. D. Harris,et al. Cellular copper transport and metabolism. , 2003, Annual review of nutrition.

[266] N. Horn. Menkes X‐linked disease: Prenatal diagnosis of hemizygous males and heterozygous females , 1981, Prenatal diagnosis.

[267] A. Rosato,et al. Solution structure and backbone dynamics of the Cu(I) and apo forms of the second metal-binding domain of the Menkes protein ATP7A. , 2004, Biochemistry.

[268] S. Lutsenko,et al. The N-terminal Metal-binding Site 2 of the Wilson's Disease Protein Plays a Key Role in the Transfer of Copper from Atox1* , 2004, Journal of Biological Chemistry.

[269] J. Markley,et al. Solution structure of the N-domain of Wilson disease protein: distinct nucleotide-binding environment and effects of disease mutations. , 2006, Proceedings of the National Academy of Sciences of the United States of America.

[270] P. Lockhart,et al. Cloning, mapping and expression analysis of the sheep Wilson disease gene homologue. , 2000, Biochimica et biophysica acta.

[271] J. Gitlin,et al. Isolation and characterization of a human liver cDNA as a candidate gene for Wilson disease. , 1993, Biochemical and biophysical research communications.

[272] S. Kaler,et al. Brachial artery aneurysms in Menkes disease. , 2006, The Journal of pediatrics.

[273] G. Ronnett,et al. Pituitary Adenylyl Cyclase-Activating Peptides and α-Amidation in Olfactory Neurogenesis and Neuronal Survival In Vitro , 2001, The Journal of Neuroscience.

[274] L. Niklason,et al. Effects of Copper and Cross-Linking on the Extracellular Matrix of Tissue-Engineered Arteries , 2005, Cell transplantation.

[275] M. Wienrich,et al. The effects of copper ions on glutamate receptors in cultured rat cortical neurons , 1996, Brain Research.

[276] I. Miyakawa,et al. Copper disposition of the fetus and placenta in a patient with untreated Wilson's disease. , 1993, American journal of obstetrics and gynecology.

[277] R. Abercrombie,et al. Luminal Ca2+ Protects against Thapsigargin Inhibition in Neuronal Endoplasmic Reticulum* , 1998, The Journal of Biological Chemistry.

[278] R. Angeletti,et al. Peptidylglycine alpha-amidating monooxygenase (PAM) in Schwann cells and glia as well as neurons. , 1990, The journal of histochemistry and cytochemistry : official journal of the Histochemistry Society.

[279] L. Braiterman,et al. Dynamics of endogenous ATP7A (Menkes protein) in intestinal epithelial cells: copper-dependent redistribution between two intracellular sites. , 2007, American journal of physiology. Gastrointestinal and liver physiology.

[280] D. Danks,et al. Copper metabolism in mottled mouse mutants: distribution of 64Cu in brindled (Mobr) mice. , 1979, The Biochemical journal.

[281] C. Rensing,et al. CopA: An Escherichia coli Cu(I)-translocating P-type ATPase. , 2000, Proceedings of the National Academy of Sciences of the United States of America.

[282] P. Ferenci. Diagnosis and current therapy of Wilson's disease , 2004 .

[283] R. Mains,et al. Developmental changes in the expression of ATP7A during a critical period in postnatal neurodevelopment , 2006, Neuroscience.

[284] I. Forgacs. GASTROENTEROLOGY , 1988, The Lancet.

[285] Analysis of the distribution of Cu, Fe and Zn and other elements in brindled mouse kidney using a scanning proton microprobe. , 1998, Journal of inorganic biochemistry.

[286] N. Kasai,et al. Direct visualization of copper-metallothionein in LEC rat kidneys: application of autofluorescence signal of copper-thiolate cluster. , 1996, The journal of histochemistry and cytochemistry : official journal of the Histochemistry Society.

[287] Torsten Herrmann,et al. Solution Structure and Intermolecular Interactions of the Third Metal-binding Domain of ATP7A, the Menkes Disease Protein* , 2006, Journal of Biological Chemistry.

[288] S. Kelleher,et al. Effects of copper supplementation on copper absorption, tissue distribution, and copper transporter expression in an infant rat model. , 2005, American journal of physiology. Gastrointestinal and liver physiology.

[289] Gary Lynch,et al. Increased spectrin proteolysis in the brindled mouse brain , 1990, Neuroscience Letters.

[290] D. Cox,et al. Copper-dependent trafficking of Wilson disease mutant ATP7B proteins. , 2000, Human molecular genetics.

[291] K. Summer,et al. Whole animal copper flux assessed by positron emission tomography in the Long – Evans cinnamon rat – a feasibility study , 2005, Biometals.

[292] E. D. Harris,et al. Copper efflux from murine microvascular cells requires expression of the menkes disease Cu-ATPase. , 1998, The Journal of nutrition.

[293] P. Nissen,et al. The Structural Basis for Coupling of Ca2+ Transport to ATP Hydrolysis by the Sarcoplasmic Reticulum Ca2+-ATPase , 2005, Journal of bioenergetics and biomembranes.

[294] J. Rommens,et al. The Wilson disease gene is a putative copper transporting P–type ATPase similar to the Menkes gene , 1993, Nature Genetics.

[295] A. Rosato,et al. An atomic-level investigation of the disease-causing A629P mutant of the Menkes protein, ATP7A. , 2005, Journal of molecular biology.

[296] D. Kosman,et al. Cuprous oxidase activity of yeast Fet3p and human ceruloplasmin: implication for function , 2003, FEBS letters.

[297] S. Kaler,et al. Distinctive Menkes disease variant with occipital horns: delineation of natural history and clinical phenotype. , 1996, American journal of medical genetics.

[298] K. Ogawa,et al. Copper‐transporting P‐type adenosine triphosphatase (ATP7B) as a cisplatin based chemoresistance marker in ovarian carcinoma: Comparative analysis with expression of MDR1, MRP1, MRP2, LRP and BCRP , 2002, International journal of cancer.

[299] J. Gitlin,et al. Functional expression of the Wilson disease protein reveals mislocalization and impaired copper-dependent trafficking of the common H1069Q mutation. , 1998, Proceedings of the National Academy of Sciences of the United States of America.

[300] M. Schilsky,et al. Biliary copper excretion capacity in intact animals: Correlation between ATP7B function, hepatic mass, and biliary copper excretion , 2000, Journal of biochemical and molecular toxicology.

[301] R. Sener. Diffusion MR imaging changes associated with Wilson disease. , 2003, AJNR. American journal of neuroradiology.

[302] H. Nazer,et al. Wilson's Disease. , 1991, Annals of Saudi medicine.

[303] L. Que,et al. Zinc Binding to the NH2-terminal Domain of the Wilson Disease Copper-transporting ATPase , 2002, The Journal of Biological Chemistry.

[304] Steven D. P. Moore,et al. Expression in Mouse Kidney of Membrane Copper Transporters Atp7a and Atp7b , 2002, Nephron.

[305] C. Keen,et al. Incorporation of copper into lysyl oxidase. , 1997, The Biochemical journal.

[306] P. Chavrier,et al. The role of ARF and Rab GTPases in membrane transport. , 1999, Current opinion in cell biology.

[307] G. Samimi,et al. Confocal Microscopic Analysis of the Interaction between Cisplatin and the Copper Transporter ATP7B in Human Ovarian Carcinoma Cells , 2004, Clinical Cancer Research.

[308] P. Lockhart,et al. The Role of GMXCXXC Metal Binding Sites in the Copper-induced Redistribution of the Menkes Protein* , 1999, The Journal of Biological Chemistry.

[309] M. Linder,et al. Copper transport to mammary gland and milk during lactation in rats. , 2002, American journal of physiology. Endocrinology and metabolism.

[310] G. Rotilio,et al. Neurodegeneration in the animal model of Menkes’ disease involves Bcl-2-linked apoptosis , 2001, Neuroscience.

[311] C. Wijmenga,et al. Identification of a new copper metabolism gene by positional cloning in a purebred dog population. , 2002, Human molecular genetics.

[312] J. Gitlin,et al. Tissue-specific ceruloplasmin gene expression in the mammary gland. , 1991, The Biochemical journal.